Antimalarial Pharmacology in Children and Pregnant Women in Uganda

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ClinicalTrials.gov Identifier: NCT01717885

Recruitment Status
:
Completed

First Posted
: October 31, 2012

Last Update Posted
: October 28, 2016

Sponsor:

University of California, San Francisco

Collaborator:

Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD)

Malaria reinfection (recrudescence or new infection) [ Time Frame: From Day 0 to 42 days of F/U when using artemether-lumefantrine for uncomplicated malaria ]

The association between PK exposure and malaria reinfection is the main secondary outcome.

Parasite clearance rate [ Time Frame: Days 0 to 42 of follow-up ]

To assess the relationship between artemisinin exposure and parasite clearance

AL and ART toxicity [ Time Frame: Days 0 to 42 of follow-up ]

To assess the relationship between artemether, lumefantrine and antiretroviral exposure and toxicity, particularly neutropenia

Original Secondary Outcome Measures

Same as current

Current Other Outcome Measures

Not Provided

Original Other Outcome Measures

Not Provided

Descriptive Information

Brief Title

Antimalarial Pharmacology in Children and Pregnant Women in Uganda

Official Title

Antimalarial Pharmacology in HIV Infected and Uninfected Children and Pregnant Women in Uganda

Brief Summary

The burden of malaria is greatest in children and pregnant women in sub-Saharan Africa. Malaria is one of the most important infectious diseases in the world. Uganda reports among the highest transmission intensities in the world. Children and pregnant women are the most vulnerable populations. HIV is also reported at high rates for these populations. If malaria and HIV require treatment at the same time, there is a high risk for drug-drug interactions. This study will:

Determine if the use of anti-HIV medications including lopinavir/ritonavir (LPV/r), nevirapine (NVP) and efavirenz (EFV) will affect the pharmacokinetic (PK) exposure of antimalarial medications (specifically artemether-lumefantrine, AL) during the treatment for uncomplicated malaria in HIV-infected children and pregnant women, and

Evaluate the impact of age and pregnancy on the PK exposure of AL.

Detailed Description

This study is designed to directly address antimalarial PK and pharmacodynamics (PD) objectives in children and pregnant women, the populations most vulnerable to malaria. This study will focus on the pharmacology of artemether-lumefantrine (AL), the most commonly prescribed anti-malarial drug in sub-Saharan Africa and inform specific dosing guidelines for AL treatment of uncomplicated malaria for these populations. Traditionally, studies have focused on non-pregnant adults, largely ignoring the effects of childhood maturation and pregnancy on drug disposition. This gap in research is specified as a top priority by the WorldWide Antimalarial Resistance Network (WWARN), who emphasize the importance of proper PK and PD study in relevant populations to reduce the threat of ACT drug resistance and treatment failure. This study will allow optimization of ACT regimens, especially in the setting of HIV co-infection and inform use of ART, specifically for the nucleoside analogues, in the setting of malaria and ACT, with the goal of reducing toxicity.

This study complements ongoing PROMOTE trials and provides valuable PK and PD data leveraged to the existing trials, greatly decreasing research costs. This study involves co-enrollment of HIV-infected children and pregnant women already enrolled in PROMOTE which is investigating PI- vs NNRTI-based ART treatment strategies for reducing malaria-related morbidity in HIV and malaria co-infected children and pregnant women. PROMOTE trials were designed in collaboration with Ugandan health care experts and officials and results are expected to rapidly impact Ugandan health policy. This study builds on knowledge gained through PROMOTE. The study also permits enrollment of HIV infected children and pregnant women not in PROMOTE but managed through TDH or other referral site in the Tororo area. Lastly this study will enroll HIV uninfected children, pregnant women and non-pregnant adults.

This study utilizes state-of-the-art PK designs and drug assay methods relying on a combination of intensive and population models to optimize PK/PD analysis. Intensive studies using serial sampling in a relatively small number of subjects will address focused questions on PK exposure while population studies using less frequent sampling in large numbers of subjects will study relationships between PK exposure, clinical response (treatment failure, new infection, and placental malaria), and toxicity (neutropenia) while considering multiple potential covariates. This study includes development and utilization of small volume assay methods for ACT and ART to optimize PK/PD study in children and pregnant women and will be a useful tool for future research trials in resource limited settings.

Rationale for this study is summarized below:

Dosing guidelines for children and pregnant women have relied on studies carried out in non-pregnant adults

Children and pregnant women exhibit distinct physiological characteristics that impact how drugs are handled by the body and thus are likely treated improperly

This gap in research has been deemed an area of high priority by WWARN • Improper dosing may compromise care of acute infection but more importantly contribute to develop of resistance

ACT therapies must be protected from factors contributing to resistance

Drug-drug interactions between anti-malarial treatment and ART must be evaluated to assure optimized dosing.

Drug toxicity, in particular neutropenia, in the setting of HIV-malaria co-infection may be due to important drug-drug interactions

Intensive PK design resulting in determination of a precise area under the concentration versus time curve (AUC) will permit robust comparisons so that results will inform treatment guidelines and policy for HIV-infected children and pregnant women.

Once optimized dosing is determined, the PK of this new dosing will be confirmed through follow-up (F/U) studies

We need state of the art analytical tools to quantitate key drugs in small volume samples collected from vulnerable populations including young children

Study Type

Observational

Study Design

Observational Model: CohortTime Perspective: Prospective

Target Follow-Up Duration

Not Provided

Biospecimen

Retention: Samples With DNA

Description:

Samples are for drug level measurements,parasite density. RNA samples are for host transcriptional and molecular markers of resistance. Samples are also retained for future use including possible genetic testing for drug metabolism variants

Sampling Method

Non-Probability Sample

Study Population

HIV infected and uninfected children and pregnant women residing in Tororo, Uganda and receiving care at local health care facilities including the Tororo District Hospital (TDH), perinatal facilities, HIV clinics and the IDRC research clinic. HIV uninfected children, pregnant women and non-pregnant adults also enrolled through TDH, perinatal facilities or other area clinics. Each participant can enroll at the time they present to one of the clinics with uncomplicated malaria

Condition

Malaria

HIV

Intervention

Not Provided

Study Groups/Cohorts

HIV+children on LPV/r

HIV+ children who are stabilized on a LPV/r based ART regimen

HIV+ children on nevirapine

HIV+ children who are stabilized on an nevirapine based ART regimen

HIV+ children on efavirenz

HIV+ children who are stabilized on an efavirenz based ART regimen

HIV+ pregnant women on LPV/r

HIV+ pregnant women who are stabilized on an LPV/r based ART regimen

HIV+ pregnant women on NVP

HIV+ pregnant women who are stabilized on an nevirapine based ART regimen

HIV+ pregnant women on EFV

HIV+ pregnant women stabilized on an efavirenz based ART regimen

HIV negative children

HIV negative children that will serve as a control for HIV positive children on either a LPV/r, NVP or EFV based ART regimen and will be compared to HIV negative non-pregnant adults

HIV negative adults

HIV negative adults that will serve as a control for comparing results to HIV negative children and HIV negative pregnant women

HIV negative pregnant women

HIV negative pregnant women who will serve as a control for HIV positive pregnant women on either a LPV/r, NVP or EFV based ART regimen and will be compared to HIV negative non-pregnant adults

Agreement to come to clinic for all follow-up clinical and PK evaluations

Provision of informed consent

HIV-INFECTED PARTICIPANTS

Children:

1) Enrollment in Promote I or meets enrollment criteria and recruited from TDH/TASO or other referral site

6 months to 8 years of age

Weight ≥6 kg

Confirmed HIV infection (positive rapid HIV test to be confirmed by Western Blot or HIV RNA after enrollment)

On a stable ART regimen for at least 10 days prior to enrollment

If co-enrolled from PROMOTE, willingness to undergo intensive PK sampling during a single episode of uncomplicated malaria, and/or population PK/parasite clearance time studies during multiple episodes of uncomplicated malaria.

If enrolled from TDH, willingness to undergo intensive PK sampling during a single episode of malaria or population PK/parasite clearance time studies during episodes of uncomplicated malaria.

Pregnant women

Enrollment in Promote Project 2 or meets enrollment criteria and recruited from TDH/TASO or other referral site

Confirmed HIV infection (positive rapid HIV test to be confirmed by Western Blot or HIV RNA after enrollment)

16 years of age or older

Estimated gestational age between 12 and 38 weeks by last menstrual period and report of quickening

Willingness to undergo intensive PK sampling during episodes of uncomplicated malaria during pregnancy.

HIV UNINFECTED PARTICIPANTS

Children:

Enrollment from TDH or other referral site

6 months to 8 years of age

Weight ≥6 kg

Confirmed HIV negative test (negative rapid HIV test to be confirmed by Western Blot or HIV RNA after enrollment)

Presentation with uncomplicated falciparum malaria as indicated by positive smear for malaria parasites along with clinical evidence of infection (fever or history of fever in the past 24 hours) with planned treatment with AL.

7) Willingness to undergo intensive PK sampling during a single episode of malaria or population PK/parasite clearance time studies during episodes of uncomplicated malaria.

Non-pregnant adults:

Age ≥ 16 years

Confirmed HIV negative test (negative rapid HIV test to be confirmed by Western Blot or HIV RNA after enrollment).

Presentation with uncomplicated falciparum malaria as indicated by positive smear for malaria parasites along with clinical evidence of infection (fever or history of fever in the past 24 hours) with planned treatment with AL.

Negative pregnancy test

Willingness to undergo intensive PK sampling during treatment for a single episode of uncomplicated malaria

Pregnant women:

Age ≥ 16 years

Confirmed HIV negative test (negative rapid HIV test to be confirmed by Western Blot or HIV RNA after enrollment)

Estimated gestational age between 12 and 38 weeks by last menstrual period and report of quickening

Presentation with uncomplicated malaria as indicated by positive smear for malaria parasites along with clinical evidence of infection (fever or history of fever in the past 24 hours) with planned treatment with AL.

No evidence of imminent delivery or threatened abortion at the time of presentation with malaria.

Willingness to undergo intensive PK sampling during episodes of uncomplicated malaria during pregnancy.

Exclusion Criteria:

History of significant comorbidities such as malignancy, active tuberculosis or other WHO stage 4 disease

Current infection with non-falciparum species

Receipt of any medications known to affect cytochrome p450 (CYP450) metabolism (except ART) within 14 days of study enrollment (see 4.2.2)